ORIGINAL ARTICLE DOI: 10.3904/kjim.2009.24.4.374
Evaluation of Ceftriaxone Utilization at Multicenter Study Hyuck Lee1, Dongsik Jung1, Joon Sup Yeom2, Jun Seong Son3, Sook-In Jung4, Yeon-Sook Kim5, Chun Kwan Kim6, Hyun-Ha Chang7, Shin-Woo Kim7, Hyun Kyun Ki8, Chi Sook Moon9, Doo Ryeon Chung10, Kyong Ran Peck10 Jae-Hoon Song10, and Gun-Jo Woo11 Department of Internal Medicine, 1Dong-A University Hospital, Busan; 2Kangbuk Samsung Hospital, Seoul; 3Kyung Hee University East-West Neo Medical Center, Seoul; 4Chonnam National University Hospital, Gwangju; 5Chungnam National University Hospital, Daejon; 6Seoul Veterans Hospital, Seoul; 7Kyungpook National University Hopital, Daegu; 8Konkuk University Hospital, Seoul; 9Inje University Paik Hospital, Busan; 10Samsung Medical Center, Seoul; 11Korea Food & Drug Administration, Seoul, Korea Background/Aims: As bacterial resistance to antimicrobial agents has grown due to the increasing use of antimicrobial agents, we sought to evaluate the suitability of ceftriaxone usage (representative of third generation cephalosporins) at 10 university hospitals in Korea. Methods: We prospectively evaluated the appropriateness of antibiotic usage in 400 adult patients who received ceftriaxone between February 1, 2006 and June 30, 2006. Drug utilization evaluation (DUE) methods were based on standards set forth by the American Society of Hospital Pharmacists. The DUE criteria used in this study were modified to be more suitable in our hospital setting: justification of drug use, critical and process indications, complications, and outcome measures. Results: The average patient age was 64.4 years. The utilization of ceftriaxone was appropriate in 262 cases (65.5%) for the justification of use, while inappropriate use was observed in 138 cases (34.5%). Common reasons for inappropriate use of ceftriaxone included continued empiric use for presumed infections, prophylactic perioperative injection, and empiric therapy for fever. Most of the critical indications showed a high rate of suitability (66.5-98.5%). Complications occurred in 37 cases (9.3%). With respect to outcome measures, clinical responses were observed in 60.7% of cases, while only 15.7% of cases showed evidence of infection eradication via negative cultures. Conclusions: Appropriate use (65.5%) of ceftriaxone was higher than inappropriate use (34.5%) at university hospitals in Korea. Inappropriate utilization, however, including continued empiric use for presumed infections and prophylactic perioperative injection remained high. Intensification of educational programs and antibiotic control systems for ceftriaxone is needed to improve the suitability of antimicrobial use. (Korean J Intern Med 2009;24:374-380) Keywords: Drug utilization review; Ceftriaxone
INTRODUCTION Bacterial resistance to antimicrobial agents due to the increasing use of antimicrobial agents has become a worldwide concern. Over the past several decades, the increased prevalence of known resistant organisms and the emergence of newly resistant organisms such as
penicillin-resistant pneumococci, methicillin-resistant Staphyloccus aureus, vancomycin-resistant enterococci, extended-spectrum beta-lactamase-producing Escherichia coli, Klebsiella pneumoniae, and imipenem-resistant gram-negative bacilli, have resulted in delays in effective therapy and the length of hospitalization, and have led to increased costs for patients [1]. Compared to infections
Received: August 22, 2008 Accepted: January 21, 2009 Correspondence to Jae-Hoon Song, M.D. Division of Infectious Diseases, Samsung Medical Center, Sungkyunkwan University College of Medicine, 50 Ilwon-dong Kangnam-gu, Seoul 135-710, Korea Tel: 82-2-3410-0320, Fax: 82-2-3410-0328, E-mail:
[email protected]
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Table 1. Criteria elements for the drug utilization evaluation of ceftriaxone No.
Elements
Exceptions
Justification of use 1
Culture and sensitivity (C&S) documented serious gram negative pulmonary infection (not pseudomonas) sensitive to ceftriaxone
Organism need not be resistant to ampicillin, and trimethoprimsulfamethoxazole if patient has documented allergy to beta-lactam antibiotics or sulfonamides
2
C&S documented acute or chronic gram negative osteomyelitis
None
Or 3
4
C&S documented meningitis due to enteric bacteria or Hemophilus influenzae Or C&S documented gonorrhea, gonococcal infection
None
None
Or 5
C&S documented pelvic inflammatory disease
None
Or 6
C&S documented chancroid
None
Or 7
C&S documented gram negative bacteremia (not pseudomonas)
None
Or 8
C&S documented serious infection due to multidrug resistant gram negative microorganism
None
Or 9
Empiric treatment of suspected gram negative bacteremia/septicemia in non-neutropenic patient or severe pneumonia
None
Or 10
Empiric treatment of suspected gram-negative non-pseudomonal meningitis
None
11
Empiric treatment of sexually acquired epididymitis
12
Appropriate C&S obtained within 48 hr before initial ceftriaxone dose
Ceftriaxone ordered in response to positive culture
13
Complete blood count (CBC) with differential obtained within 48 hr before initial ceftriaxone dose
None
14
Serum creatinine (SCr) concentration or urinary creatinine clearance (CrCl) obtained if severe hepatic and renal impairment occurs
If severe hepatic and renal impairment, total daily dose lower than or equal to 2 g
15
Liver function tests [total serum bilirubin, alkaline phosphatase (ALP), aspartate aminotransferase (AST), and alanine aminotransferase (ALT)] obtained within 7 days before initial ceftriaxone dose
None
16
Previous hypersensitivity reaction to beta-lactam antibiotics NOT noted in patient’s chart
None
17
Appropriate ceftriaxone dosage; (a) uncomplicated gonorrhea/gonococcal infection: 250 mg IM single dose (b) disseminated gonorrhea/gonococcal infection: 1 g IV q 24 hr for 7 days (c) pelvic inflammatory disease: 250 mg IM as a single dose followed by doxycycline (d) sexually acquired epididymitis: 250 mg IM as a single dose followed by doxycycline (e) chancroid : 250 mg IM as a single dose (f) moderate infection: 1-2 g IV/IM q 24 hr (g) severe infection: 1 g IV/IM q 12 hr or 2g IV/IM q 24 hr
None
Or None
Critical (process) indicators
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No.
Elements
Exceptions
18
Vital signs monitored at least three times daily (i.e., once each nursing shift) until patient becomes afebrile and at least one daily thereafter during ceftriaxone therapy
None
19
White blood cell (WBC) count obtained at least once weekly during ceftriaxone therapy
None
20
SCr or urinary CrCl obtained at least once weekly during ceftriaxone therapy
None
21
Appropriate treatment duration: 7-14 days
None
22
Anaphylaxis: breathing difficulty, wheezing, laryngeal edema, flushing, tarchycardia, and/or hypotension
Discontinue ceftriaxone Treat symptomatically with epinephrine or antihistamine with or with or without supportive care, e.g., fluids, cardiopulmonary resuscitation, and assisted ventilation Use alternative anti-infective therapy
23
Cutaneous reactions: urticaria, angioedema, maculopapular eruptions, pruritus, erythema multiforme, and/or Stevens-Johnson syndrome
Identify other drug and nondrug causes If mild reaction, treat symptomatically with antihistamine or corticosteroid; pretreat with antihistamine or corticosteroid for subsequent doses If severe reaction, discontinue ceftriaxone; treat symptomatically with epinephrine or antihistamine with or without supportive care, including cardiopulmonary resuscitation and assisted ventilation; use alternative anti-infective therapy
24
Superinfection; overgrowth of another organism (e.g., Enterococcus, Candida, Pseudomonas, or Acinetobacter species)
Discontinue ceftriaxone and treat primary infection with alternative antimicrobial if possible Begin appropriate anti-infective therapy for superinfection
25
Gastrointestinal effects: nausea, dyspepsia, diarrhea, constipation, vomiting, abdominal pain or discomfort, oral ulceration, dysphagia, intestinal perforation, ileus, dry mouth, and/or gastrointestinal bleeding
Identify other drug and nondrug causes Provide symptomatic care and supportive therapy If mild reaction, decrease dosage If severe reaction, discontinue ceftriaxone and switch to alternative anti-infective therapy
26
Bad taste
Identify other drug and nondrug causes If mild reaction, decrease dosage If severe reaction, discontinue ceftriaxone and switch to alternative anti-infective therapy
27
Antimicrobial-associated pseudomembranous colitis (AAPMS) characterized by at least two of the following: (a) fever, diarrhea, abdominal pain, or ileus (b) proctoscopy or colonoscopy revealing yellow-white exudative plaques or pseudomembranes (c) biopsy showing histologic changes consistent with AAPMS (d) fecal leukocytes (e) positive culture for Clostridium difficile with or without positive C. difficile tox
Identify and discontinue causative agent and use alternative anti-infective therapy if possible Replace fluid and electrolyte losses with IV or oral therapy if nothingby-mouth order is discontinued Initiate therapy per severity of condition: IV metronidazole for patient with nothing-by-mouth orders ; or oral vancomycin, metronidazole, or bacitracin, each with or without anion-exchange resin, if nothing-bymouth order is discontinued 22-24 hr
28
Neurologic effects: peripheral neuropathy manifested as paresthesia, numbness or ataxia, and/or incoordination or convulsion
Identify other drug and nondrug causes Discontinue ceftriaxone and treat symptomatically; use alternative anti-infective therapy
29
Central nervous system effects: drowsiness, fatigue, malaise, lethargy, psychosis, depression, mania, phobia, confusion, hallucinations, dizziness, lightheadedness, anxiety, tremor, and/or insomnia
Identify other drug and nondrug causes If mild reaction, treat symptomatically If severe or intolerable reaction, discontinue ceftriaxone and treat symptomatically; use alternative anti-infective therapy
30
Hepatotoxicity as measured by liver function tests (at least two times upper limit of normal) for one or more of the following: ALT, AST, ALP, lactate dehydrogenase, and bilirubin; or clinical symptoms of liver disease (e.g., right upper quadrant pain or tenderness, jaundice, nausea, and vomiting)
(e.g., right upper quadrant pain or tenderness, jaundice, nausea, and vomiting) Identify other drug and nondrug causes Discontinue ceftriaxone and switch to alternative anti-infective therapy Monitor liver enzymes at least twice weekly until values return to normal or to patient’s baseline
None
Complications
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No.
Elements
Exceptions
31
Bleeding disturbances: thrombocytopenia (platelet count < 70,000/mm3) or Thrombocytosis (platelet count > 400,000/mm3)
Identify other drug and discontinue ceftriaxone Use alternative anti-infective therapy Provide supportive care and symptomatic therapy; monitor PT, activated partial thromboplastin time, and platelet count at least twice weekly
32
Nonbleeding-related hematologic effects: leukopenia (leukocyte count < 500/mm3), eosinophilia (absolute eosinophil count > 500/mm3), or pancytopenia
Identify other drug and nondrug causes Discontinue ceftriaxone. Use alternative anti-infective therapy Provide supportive care and symptomatic therapy; monitor CBC with differential daily
33
Local effects of IV therapy: phlebitis, burning, pain and inflammation, Identify other drug and nondrug causes erythema, pruritus, paresthesia, and/or swelling If mild reaction, treat symptomatically; consider alternative IV site in a larger vein and increase drug dilution to 1 mg/mL If severe reaction, discontinue infusion and remove IV catheter; use alternative anti-infective therapy
34
Eradication of infection as evidenced by negative (sterile) cultures 72 hours after discontinuation of ceftriaxone
Outcome measures New organism or another infection identified, clinical cure determined by absence of erythema and tenderness at affected site Patient discharged and unavailable for follow up patient expired Patient discharged before therapy completed
Or 35
Fever reduction (decrease of at least 1˚C from peak temperature) within 3 days of initial ceftriaxone dose
Fever not present initially Another cause of elevated temperature known or suspected new source of infection known or suspected Patient expired
Or 36
WBC count within normal limits (3.7-9.4 × 109/mm3)
WBC count not elevated prior to therapy Patient neutropenic prior to therapy Another cause of elevated WBC count known or suspected Patient expired
Or 37
Clinical improvement noted in progress
caused by susceptible pathogens, those caused by resistant pathogens are associated with higher rates of morbidity and mortality [2,3]. Furthermore, antimicrobial drug resistance has been projected to add between $100 million and $30 billion annually to health-care costs [4]. During the past several years, the problem of antibiotic resistance has noticeably worsened in Korea [5]. With gradual increases in expensive antimicrobial agents, the cost of antimicrobial agents relative to total medical insurance expenses has reached 33.1% [6]. When considering that misuse of antimicrobial agents is the most important cause of antibiotic resistance, the logical first step is to evaluate the suitability of antibiotic usage. Only one usage analysis of cephalosporins and aminoglycosides for surgical prophylaxis has been conducted at
New organism or another infection suspected or identified Patient discharged before therapy completed and unavailable for follow-up Patient expired
a university hospital in Korea, and most reports examining the appropriateness of antibiotic use have been individual studies [7-12]. Antibiotic use evaluations are a basic measure for evaluating the appropriate usage of antimicrobial agents; however, data gathered from individual hospitals have limited benefits for policy-making. For this reason, we examined antibiotic use status and evaluated the appropriateness of the antibiotic usage in 10 university hospitals in Korea. Specifically, in the present study, we evaluated the use of a specific antibiotic (ceftriaxone, a representative of third-generation cephalosporin) and attempted to compile basic data outlining the appropriate use of antibiotics.
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Table 2. Distribution of ceftriaxone daily dosage Daily dosage (g/day) 1.0
1.5-2.0
2.0
2.0-2.5
3.0
4.0
Total
9 (2.2%)
2 (0.5%)
340 (85.3%)
1 (0.3%)
8 (2.0%)
40 (10.0%)
400 (100%)
Table 3. Causes of inappropriate ceftriaxone use Cause
Values (n=138)
Routine perioperative prophylaxis
69 (50)
Inappropriate empiric therapy (>5 days) for
48 (34.8)
presumed infections Systemic prophylaxis for infection or colonization Figure 1. Justification of the use of ceftriaxone.
METHODS The criteria used for antibiotic selection included the following: antibiotics with a risk of abuse, those that were being used in high amounts in Korean hospitals, antibiotics that were likely causing resistance due to increased usage, and those that were not being controlled by an antibiotic prescribing restriction system. Ceftriaxone, a broadspectrum parenteral cephalosporin, was selected as representative of unrestricted antibiotics. A drug utilization evaluation (DUE) was conducted to determine whether ceftriaxone was being used appropriately based on the “Criteria for Drug Use Evaluation” of the American Society of Hospital Pharmacists [13]. The criteria for DUE used in this study were modified based on their suitability in the Korean hospital setting: justification of drug use, critical and process indications, complications, and outcome measures. A DUE was performed prospectively by reviewing medical records for a total of 400 patients (10 hospitals with 40 patients each) who received ceftriaxone during hospitalization between February 1, 2006 and June 30, 2006, and these data were used in this study. Medical records were examined for the diagnosis, the reason for initiating and discontinuing therapy, gender, dose, frequency of administration, culture and sensitivity (C&S) results, renal function, and duration of antibiotic therapy. All medical records were examined for compliance to the clinical indicators listed above. Indications for which ceftriaxone was deemed either acceptable or unacceptable are shown in Table 1. Any patients for whom therapy was deemed unacceptable
21 (15.2)
Values are number (%).
were reviewed with criteria established at the onset of the DUE. Enrolled hospitals were Dong-A University Hospital, Kangbuk Samsung Hospital, Samsung Medical Center, Chungbuk National University Hospital, Chonnam National University Hospital, Chungnam National University Hospital, Seoul Veterans Hospital, Kyungpook National University Hospital, Konkuk University Hospital, and Inje University Paik Hospital.
RESULTS In total, 400 patients (247 men, 153 women) with a mean age of 64.4 years (range, 3 to 93; 95% CI, 32.4 to 96.4) were reviewed, with 10 cases at each of the 10 institutions. Most cases involved the department of internal medicine (58%); the remainders were in neurosurgery (12%), surgery (7.5%), orthopedic surgery (3.7%), thoracic surgery (3.7%), urology (2.7%), otolaryngology (2%), neurology (2%), and others (4.3%). Ceftriaxone dosing regimens are presented in Table 2. In 340 cases (85%), ceftriaxone was dosed as 2 g/day (range, 1 to 4). The mean duration of ceftriaxone use was 10.3 days (range, 1 to 61).
Justification of ceftriaxone use The use of ceftriaxone was appropriate in 262 cases (65.5%), and inappropriate in 138 cases (34.5%; Fig. 1). The causes of inappropriate ceftriaxone use included routine perioperative prophylaxis (50%), inappropriate empirical therapy (>5 days) for presumed infections (34.8%), and systemic prophylaxis for infection or
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Table 4. Ceftriaxone drug utilization evaluation: critical (process) indicators Criteria
Accepted level
Unaccepted level
Appropriate cultures and sensitivities obtained within 48 hr before initial ceftriaxone dose
266 (66.5)
134 (33.5)
Complete blood count with differential obtained within 48 hr before initial ceftriaxone dose
371 (92.7)
29 (7.3)
Liver function test obtained within 7 days before initial ceftriaxone dose
382 (95.5)
18 (4.5)
Previous hypersensitivity reaction to beta-lactam antibiotics NOT noted in patient’s chart
394 (98.5)
6 (1.5)
Appropriate ceftriaxone dosage
337 (84.2)
63 (15.8)
White blood cell count obtained at least 1/wk during therapy
379 (94.7)
21 (5.3)
Vital signs monitored at least three times daily
386 (96.5)
14 (3.5)
Serum creatinine (sCr) monitored at least 2/wk during therapy if baseline sCr within normal limit
376 (94)
Duration of therapy
229 (57.2)
24 (6) 171 (42.8)
Values are frequency (%).
Table 5. Ceftriaxone drug utilization evaluation: complications Complication
Value (n=37)
Hepatotoxicity
16 (43.2)
GI trouble
12 (32.4)
Cutaneous reaction (e.g., skin rash)
6 (16.2)
Bleeding disturbance
2 (5.5)
Peripheral neuropathy
1 (2.7)
Values are number (%).
colonization (15.2%, Table 3).
Critical (process) indicators Most of the critical and process indications showed high rates of appropriateness (84.2-98.5%), excluding inappropriate C&S tests prior to the initial ceftriaxone dose (33.5%) and inappropriate duration of therapy (42.8%, Table 4).
Complications Hepatotoxicity occurred in 16 cases (43.2%), gastrointestinal trouble in 12 cases (32.4%), cutaneous reaction in 6 cases (16.2%), bleeding disturbances in 2 cases (5.5%), and peripheral neuropathy in 1 case (2.7%, Table 5). Each case was managed appropriately.
Outcome measures Clinical improvement was noted in 243 patients (60.7%), while documentation of microbiological eradication evidenced by negative cultures 72 hours after discontinuation of ceftriaxone was inappropriate in 337 patients (84.3%).
DISCUSSION The goal of antibiotic therapy is to achieve the best possible clinical outcomes while consuming the least amount of hospital resources. Health-care systems are under intense pressure to increase the quality of care and at the same time reduce costs. Pressure to reduce the cost of antimicrobial therapy is especially intense because these drugs may account for a large portion of a hospital’s pharmacy budget. According to previous investigations on antibiotic use, antibiotics might account for 33.1% of the medical insurance budget in Korea, and 20-50% of these cases are suspected to have been abuse [6]. In many cases, antibiotics were prescribed for prophylaxis rather than for treatment [6,7]. Antibiotic abuse such as this in the community and hospitals fuels the crisis of antibiotic resistance, which ultimately results in virtually all pathogenic bacteria becoming resistant to older antibiotics. During the past several years, the problem of antibiotic resistance has noticeably worsened in Korea [5]. We performed a DUE for a specific antibiotic and attempted to gather basic data to examine the appropriate use of antibiotics. Furthermore, we sought to prevent antibiotic misuse and reduce unnecessary medical costs. The one limitation of previous studies for DUE is that most were retrospective and focused on a specific department. To overcome this problem, we prospectively evaluated the appropriate use of ceftriaxone usage (representative of thirdgeneration cephalosporins) at 10 university hospitals in Korea. Ceftriaxone is major drug that is used in the treatment of many important infections due to its high antibacterial potency, wide spectrum of activity, and low potential for toxicity. Its superior activity against Enterobacteriaceae, however, is being challenged by the
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increasing frequency of beta-lactamase-mediated resistance. Kim et al. [8] reported that 47% of cases met the criteria for justified use in a retrospective study at a university hospital in 1999. In contrast, our study showed that the appropriate use of ceftriaxone was relatively higher (65.5%) as compared to other studies. This difference may be attributable to the fact that the justification of use criteria were stricter and our study allowed more acceptable cases for empirical therapy. Although the appropriateness (65.5%) of ceftriaxone usage was higher than inappropriateness (34.5%) in tertiary care hospitals in Korea, unsuitable utilization such as continued empiric use for presumed infections and prophylactic perioperative injection remained high. Furthermore, appropriate selection of an antibiotic according to C&S was relatively low. Of the critical indications, a lack of C&S prior to initial ceftriaxone dose and an inappropriate duration of therapy were most common. Others showed quite high rates of appropriateness (84.298.5%, Table 4). Ceftriaxone is considered to be low in side effects. Among the complications, hepatotoxicity (16 cases, 4%) and GI difficulties (12 cases, 3%) were most common (Table 5). Each case was managed appropriately. Outcome analyses showed a relatively high clinical improvement rate of 60.7%, while microbiological documentation by follow-up culture was poor (84.3%). These results show that ceftriaxone, when used empirically, should be reevaluated within 72 hours of initiating therapy and when C&S data are reported. Therapy should be discontinued if the C&S report demonstrates that the organisms are sensitive to equally efficacious, less costly antibiotics. According to data generated by this DUE, a combination of physician education programs and feedback control systems directed toward rational ceftriaxone use is suggested for proper medical treatment.
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